| Literature DB >> 29251086 |
Xu Liu1, Lixin Cong2, Chunmei Wang1, He Li1, Chengyi Zhang1, Xingang Guan3, Peng Liu3, Yu Xie3, Jianguang Chen1, Jinghui Sun1.
Abstract
1. Schizandrol A is an active component in schisandra, also the representative component for the identification of schisandra. 2. A rapid resolution liquid chromatography coupled with quadruple-time-of-flight mass spectrometry (RRLC-QTOF/MS) was developed to investigate the pharmacokinetics of schizandrol A after its intragastric administration (50 mg/kg) in rats. 3. Schizandrol A was rapidly absorbed (T max = 2.07 h), with a longer duration (t 1/2 = 9.48 h) and larger apparent volume of distribution (Vz/F = 111.81 l/kg) in rats. Schizandrol A can be detected in main organs and the order of its distribution was in the liver > kidney > heart > spleen > brain, particularly higher in the liver. 4. Five schizandrol A metabolites were identified, including 2-demethyl-8(R)-hydroxyl-schizandrin, 3-demethyl-8(R)-hydroxyl-schizandrin, hydroxyl-schizandrin, demethoxy-schizandrin, 2, 3-demethyl-8(R)-hydroxyl-schizandrin, indicating that the hydroxylation and demethylation may be the major metabolic way of schizandrol A. 5. This study defined the pharmacokinetic characteristics of schizandrol A in vivo, and the RRLC-QTOF/MS is more sensitive and less limited by conditions, and needs less samples, which may be a useful resource for the further research and development of schisandrol A.Entities:
Keywords: RRLC–QTOF/MS; Schizandrol A; distribution; metabolite; pharmacokinetics
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Year: 2019 PMID: 29251086 DOI: 10.1080/00498254.2017.1418543
Source DB: PubMed Journal: Xenobiotica ISSN: 0049-8254 Impact factor: 1.908